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Genetic evidence supporting the association of protease and protease inhibitor genes with inflammatory bowel disease: a systematic review

cris.virtualsource.author-orcid27e66509-69e4-4bbf-ab62-ebd20b6d2e74
cris.virtualsource.author-orcidc0dd548b-3615-470c-8476-aa9a40d49236
cris.virtualsource.author-orcid13229807-efc9-46b7-a314-304594390461
cris.virtualsource.author-orcide011d6de-b8e1-4d81-80b0-b19bf77501dd
datacite.rightsopen.access
dc.contributor.authorJüni, Peter
dc.contributor.authorJüni, Peter
dc.contributor.authorBekkering, Geertruida E
dc.contributor.authorNüesch, Eveline
dc.contributor.authorMendes, Camila T
dc.contributor.authorSchmied, Stefanie
dc.contributor.authorWyder, Stefan
dc.contributor.authorKellen, Eliane
dc.contributor.authorVilliger, Peter
dc.contributor.authorRutgeerts, Paul
dc.contributor.authorVermeire, Séverine
dc.contributor.authorLottaz, Daniel
dc.date.accessioned2024-10-11T09:22:21Z
dc.date.available2024-10-11T09:22:21Z
dc.date.issued2011
dc.description.abstractAs part of the European research consortium IBDase, we addressed the role of proteases and protease inhibitors (P/PIs) in inflammatory bowel disease (IBD), characterized by chronic mucosal inflammation of the gastrointestinal tract, which affects 2.2 million people in Europe and 1.4 million people in North America. We systematically reviewed all published genetic studies on populations of European ancestry (67 studies on Crohn's disease [CD] and 37 studies on ulcerative colitis [UC]) to identify critical genomic regions associated with IBD. We developed a computer algorithm to map the 807 P/PI genes with exact genomic locations listed in the MEROPS database of peptidases onto these critical regions and to rank P/PI genes according to the accumulated evidence for their association with CD and UC. 82 P/PI genes (75 coding for proteases and 7 coding for protease inhibitors) were retained for CD based on the accumulated evidence. The cylindromatosis/turban tumor syndrome gene (CYLD) on chromosome 16 ranked highest, followed by acylaminoacyl-peptidase (APEH), dystroglycan (DAG1), macrophage-stimulating protein (MST1) and ubiquitin-specific peptidase 4 (USP4), all located on chromosome 3. For UC, 18 P/PI genes were retained (14 proteases and 4 protease inhibitors), with a considerably lower amount of accumulated evidence. The ranking of P/PI genes as established in this systematic review is currently used to guide validation studies of candidate P/PI genes, and their functional characterization in interdisciplinary mechanistic studies in vitro and in vivo as part of IBDase. The approach used here overcomes some of the problems encountered when subjectively selecting genes for further evaluation and could be applied to any complex disease and gene family.
dc.description.numberOfPages1
dc.description.sponsorship
dc.description.sponsorshipUniversitätsklinik für Rheumatologie, klinische Immunologie und Allergologie
dc.description.sponsorshipInstitut für Sozial- und Präventivmedizin (ISPM)
dc.identifier.doi10.7892/boris.7358
dc.identifier.isi000294802800024
dc.identifier.pmid21931648
dc.identifier.publisherDOI10.1371/journal.pone.0024106
dc.identifier.urihttps://boris-portal.unibe.ch/handle/20.500.12422/77813
dc.language.isoen
dc.publisherPublic Library of Science
dc.publisher.placeLawrence, Kans.
dc.relation.ispartofPLoS ONE
dc.relation.issn1932-6203
dc.relation.organizationDCD5A442BECFE17DE0405C82790C4DE2
dc.relation.organizationDCD5A442BC43E17DE0405C82790C4DE2
dc.relation.organizationDCD5A442BAD8E17DE0405C82790C4DE2
dc.titleGenetic evidence supporting the association of protease and protease inhibitor genes with inflammatory bowel disease: a systematic review
dc.typearticle
dspace.entity.typePublication
dspace.file.typetext
oaire.citation.issue9
oaire.citation.startPagee24106
oaire.citation.volume6
oairecerif.author.affiliationInstitut für Sozial- und Präventivmedizin (ISPM)
oairecerif.author.affiliationInstitut für Sozial- und Präventivmedizin (ISPM)
oairecerif.author.affiliation
oairecerif.author.affiliationUniversitätsklinik für Rheumatologie, klinische Immunologie und Allergologie
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unibe.description.ispublishedpub
unibe.eprints.legacyId7358
unibe.journal.abbrevTitlePLOS ONE
unibe.refereedtrue
unibe.subtype.articlejournal

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